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首页> 外文期刊>Breast cancer online: BCO >Review of: c-Myc suppresses p21WAF1/CIP1 expression during oestrogen signalling and antioestrogen resistance in human breast cancer cells
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Review of: c-Myc suppresses p21WAF1/CIP1 expression during oestrogen signalling and antioestrogen resistance in human breast cancer cells

机译:c-Myc抑制人乳腺癌细胞雌激素信号传导和抗雌激素抵抗过程中p21WAF1 / CIP1表达

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Citation of original article:S. Mukherjee, S. E. Conrad. Journal of Biological Chemistry 2005; 280: 17616–17625.Abstract of the original article:Oestrogen rapidly induces expression of the proto-oncogene c-Myc. c-Myc is required for oestrogen-stimulated proliferation of breast cancer cells, and deregulated c-Myc expression has been implicated in antioestrogen resistance. In this report, we investigate the mechanism(s) by which c-Myc mediates oestrogen-stimulated proliferation and contributes to cell cycle progression in the presence of antioestrogen. The MCF-7 cell line is a model of oestrogen-dependent, antioestrogen-sensitive human breast cancer. Using stable MCF-7 derivatives with inducible c-Myc expression, we demonstrated that in antioestrogen-treated cells, the elevated mRNA and protein levels of p21WAF1/CIP1, a cell cycle inhibitor, decreased upon either c-Myc induction or oestrogen treatment. Expression of p21 blocked c-Myc-mediated cell cycle progression in the presence of antioestrogen, suggesting that the decrease in p21WAF1/CIP1 is necessary for this process. Using RNA interference to suppress c-Myc expression, we further established that c-Myc is required for oestrogen-mediated decreases in p21WAF1/CIP1. Finally, we observed that neither c-Myc nor p21WAF1/CIP1 is regulated by oestrogen or antioestrogen in an antioestrogen-resistant MCF-7 derivative. The p21 levels in the antioestrogen-resistant cells increased when c-Myc expression was suppressed, suggesting that loss of p21 regulation was a consequence of constitutive c-Myc expression. Together, these studies implicate p21WAF1/CIP1 as an important target of c-Myc in breast cancer cells and provide a link between oestrogen, c-Myc, and the cell cycle machinery. They further suggest that aberrant c-Myc expression, which is frequently observed in human breast cancers, can contribute to antioestrogen resistance by altering p21WAF1/CIP1 regulation.
机译:引用原始文章:S。 Mukherjee,S。E. Conrad。生物化学杂志2005; 280:17616–17625。原始文章的摘要:Oestrogen快速诱导原癌基因c-Myc的表达。 c-Myc是雌激素刺激的乳腺癌细胞增殖所必需的,而c-Myc表达失调与抗雌激素抵抗有关。在本报告中,我们研究了c-Myc介导雌激素刺激的增殖并在存在抗雌激素的情况下促进细胞周期进程的机制。 MCF-7细胞系是雌激素依赖性,抗雌激素敏感的人类乳腺癌的模型。使用具有可诱导的c-Myc表达的稳定MCF-7衍生物,我们证明了在抗雌激素处理的细胞中,细胞周期抑制剂p21WAF1 / CIP1的mRNA和蛋白质水平升高,在c-Myc诱导或雌激素处理后均降低。在存在抗雌激素的情况下,p21的表达阻断了c-Myc介导的细胞周期进程,这表明p21WAF1 / CIP1的减少对于该过程是必要的。使用RNA干扰抑制c-Myc表达,我们进一步确定c-Myc是雌激素介导的p21WAF1 / CIP1减少所必需的。最后,我们观察到在抗雌激素耐药的MCF-7衍生物中,c-Myc和p21WAF1 / CIP1均不受雌激素或抗雌激素的调节。当抑制c-Myc表达时,抗雌激素抵抗细胞中的p21水平升高,表明p21调控的丧失是组成性c-Myc表达的结果。总之,这些研究暗示p21WAF1 / CIP1是乳腺癌细胞中c-Myc的重要靶标,并提供了雌激素,c-Myc与细胞周期机制之间的联系。他们进一步表明,在人类乳腺癌中经常观察到的异常c-Myc表达可以通过改变p21WAF1 / CIP1调节来促进抗雌激素抵抗。

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